Pain Clinical Trial
Official title:
Clinical Pharmacogenetic of Ibuprofen Enantiomers After Lower Third Molar Surgeries
The present clinical trial randomized will be to assess the link between the different haplotypes of CYP2C8 and CYP2C9 genes and the clinical efficacy of ibuprofen after lower third molar extractions. Onset, duration of postoperative analgesia, duration of anesthetic action on soft tissues, intraoperative bleeding, hemodynamic parameters, postoperative mouth opening and wound healing at the 7th postoperative day were evaluated. For this purpose, 200 healthy volunteers underwent removal of one lower third molar, under local anesthesia with articaine 4% (1:200,000 adrenaline) will be genotyped and phenotyped for these genes and their postoperative records with all data collected will be compared with the haplotypes found in the Brazilian population.
The aim of this study will be to assess the link between the different haplotypes of CYP2C8
and CYP2C9 genes and the clinical efficacy of ibuprofen after lower third molar extractions
regarding pain, swelling and trismus, adverse reactions, the amount of pain medication used,
the patient satisfaction with the drug and the influence of the ability on preoperative
modulation of conditioned pain. We will evaluate also the relationship between the different
haplotypes of OPRM1 gene (SNP A118G), the salivary concentrations of pro-inflammatory
cytokines (IL-2, IL-4, IL-6, IL-10 and TNF-±), and preoperative conditioned pain modulation.
Therefore, 200 patients will be genotyped and phenotyped for these genes and their
postoperative records with all data collected will be compared with the haplotypes found in
the Brazilian population.
For analysis of the proposed genes, saliva will be collected, which will serve as a source of
genomic DNA. For molecular analysis it will be performed polymerase chain reaction (PCR). All
tests will be conducted and validated by Applied Biosystems®. Also it will be held in the
research, genetic sequencing of the genes CYP2C8, CYP2C9 and OPRM1, to verify possible
correlations of these genes with postoperative pain and pain modulation.
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